Literature DB >> 33585480

Is Senescence-Associated β-Galactosidase a Reliable in vivo Marker of Cellular Senescence During Embryonic Development?

José Antonio de Mera-Rodríguez1, Guadalupe Álvarez-Hernán1, Yolanda Gañán2, Gervasio Martín-Partido1, Joaquín Rodríguez-León2, Javier Francisco-Morcillo1.   

Abstract

During vertebrate embryonic development, cellular senescence occurs at multiple locations. To date, it has been accepted that when there has been induction of senescence in an embryonic tissue, β-galactosidase activity is detectable at a pH as high as 6.0, and this has been extensively used as a marker of cellular senescence in vivo in both whole-mount and cryosections. Such senescence-associated β-galactosidase (SA-GAL) labeling appears enhanced in degenerating regions of the vertebrate embryo that are also affected by programmed cell death. In this sense, there is a strong SA-GAL signal which overlaps with the pattern of cell death in the interdigital tissue of the developing limbs, and indeed, many of the labeled cells detected go on to subsequently undergo apoptosis. However, it has been reported that β-GAL activity at pH 6.0 is also enhanced in healthy neurons, and some retinal neurons are strongly labeled with this histochemical technique when they begin to differentiate during early embryonic development. These labeled early post-mitotic neurons also express other senescence markers such as p21. Therefore, the reliability of this histochemical technique in studying senescence in cells such as neurons that undergo prolonged and irreversible cell-cycle arrest is questionable because it is also expressed in healthy post-mitotic cells. The identification of new biomarkers of cellular senescence would, in combination with established markers, increase the specificity and efficiency of detecting cellular senescence in embryonic and healthy mature tissues.
Copyright © 2021 de Mera-Rodríguez, Álvarez-Hernán, Gañán, Martín-Partido, Rodríguez-León and Francisco-Morcillo.

Entities:  

Keywords:  cell death; cell senescence; development; histochemistry; limb; retina

Year:  2021        PMID: 33585480      PMCID: PMC7876289          DOI: 10.3389/fcell.2021.623175

Source DB:  PubMed          Journal:  Front Cell Dev Biol        ISSN: 2296-634X


  97 in total

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Authors:  Alexandra Bernadotte; Victor M Mikhelson; Irina M Spivak
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9.  Postmitotic neurons develop a p21-dependent senescence-like phenotype driven by a DNA damage response.

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  15 in total

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Review 5.  Untangling senescent and damage-associated microglia in the aging and diseased brain.

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6.  Analysis of Programmed Cell Death and Senescence Markers in the Developing Retina of an Altricial Bird Species.

Authors:  Guadalupe Álvarez-Hernán; José Antonio de Mera-Rodríguez; Ismael Hernández-Núñez; Alfonso Marzal; Yolanda Gañán; Gervasio Martín-Partido; Joaquín Rodríguez-León; Javier Francisco-Morcillo
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Review 9.  Senescence-Induced Chemoresistance in Triple Negative Breast Cancer and Evolution-Based Treatment Strategies.

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10.  Endogenous pH 6.0 β-Galactosidase Activity Is Linked to Neuronal Differentiation in the Olfactory Epithelium.

Authors:  José Antonio de Mera-Rodríguez; Guadalupe Álvarez-Hernán; Yolanda Gañán; Ana Santos-Almeida; Gervasio Martín-Partido; Joaquín Rodríguez-León; Javier Francisco-Morcillo
Journal:  Cells       Date:  2022-01-16       Impact factor: 6.600

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